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首页> 外文期刊>Veterinary Pathology >Pathology of the Emerging Mycobacterium tuberculosis Complex Pathogen, Mycobacterium mungi, in the Banded Mongoose (Mungos mungo)
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Pathology of the Emerging Mycobacterium tuberculosis Complex Pathogen, Mycobacterium mungi, in the Banded Mongoose (Mungos mungo)

机译:新出现的分枝杆菌结核分枝杆菌复合病原体,分枝杆菌骨膜术(Mungos Mungo)

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Wild banded mongooses (Mungos mungo) in northeastern Botswana and northwest Zimbabwe are infected with a novel Mycobacterium tuberculosis complex (MTC) pathogen, Mycobacterium mungi. We evaluated gross and histologic lesions in 62 infected mongooses (1999-2017). Many tissues contained multifocal irregular, lymphohistiocytic to granulomatous infiltrates and/or multifocal or coalescing noncaseating to caseating granulomas with variable numbers of intralesional acid-fast bacilli. Over one-third of nasal turbinates examined had submucosal lymphohistiocytic to granulomatous infiltrates, erosion and ulceration of the nasal mucosa, bony remodeling, and nasal distortion. Similar inflammatory cell infiltrates expanded the dermis of the nasal planum with frequent ulceration. However, even in cases with intact epidermis, acid-fast bacilli were present in variable numbers among dermal infiltrates and on the epidermal surface among desquamated cells and debris, most commonly in small crevices or folds. In general, tissue involvement varied among cases but was highest in lymph nodes (50/54, 93%), liver (39/53, 74%), spleen (37/51, 73%), and anal glands/sacs (6/8, 75%). Pulmonary lesions were present in 67% of sampled mongooses (35/52) but only in advanced disseminated disease. The pathological presentation of M. mungi in the banded mongoose is consistent with pathogen shedding occurring through scent-marking behaviors (urine and anal gland secretions) with new infections arising from contact with these contaminated olfactory secretions and percutaneous movement of the pathogen through breaks in the skin, nasal planum, and/or skin of the snout. Given the character and distribution of lesions and the presence of intracellular acid-fast bacilli, we hypothesize that pathogen spread occurs within the body through a hematogenous and/or lymphatic route. Features of prototypical granulomas such as multinucleated giant cells and peripheral fibrosis were rarely present in affected mongooses. Acid-fast bacilli were consistently found intracellularly, even in regions of necrosis. The mongoose genome has a unique deletion (RDImon) that includes part of the encoding region for PPE68 (Rv3873), a gene co-operonic with PE35. These proteins can influence the host's cellular immune response to mycobacterial infections, and it remains uncertain how this deletion might contribute to observed patterns of pathology. M. mungi infection in banded mongooses is characterized by both a unique transmission and exposure route, as well as accompanying pathological features, providing an opportunity to increase our understanding of MTC pathogenesis across host-pathogen systems.
机译:狂野带状猫鼬(Mungos Mungo)在东北博茨瓦纳和西北津巴布韦被感染了一种新的结核分枝杆菌复合物(MTC)病原体,Mungium。我们在62名感染的咒语中评估了总体和组织学病变(1999-2017)。许多组织含有多焦点不规则的,淋巴管霉菌,肉芽肿渗透和/或多焦点或聚合的非加入非划分,以具有可变数量的鳞片内酸快速杆菌的颗粒颗粒组织。在鼻内鼻内鼻内鼻内鼻内鼻内鼻腔淋巴化合物,鼻粘膜,鼻粘膜,骨质重塑和鼻部畸变的肿瘤淋巴管蛋白酶有粘糊糊的淋巴管蛋白酶。类似的炎症细胞渗透频繁溃疡地扩增了鼻PALPUM的真皮。然而,即使在具有完整表皮的情况下,酸快速杆菌也存在于真皮浸润的可变数中,并且在脱皮细胞和碎片中的表皮表面上存在,最常见于小裂缝或褶皱。一般而言,组织受累变化,但在淋巴结(50/54,93%),肝脏(39/53,74%),脾脏(37/51,73%)和肛门腺/囊中(6 / 8,75%)。肺病变存在于67%的采样的猫鼬(35/52)中,但仅在晚期散发疾病中。带状猫鼬中的M. mungi的病理介绍与通过气味标记行为(尿液和肛门腺分泌物)发生的病原体脱落,其具有与这些受污染的嗅觉分泌物接触产生的新感染和病原体通过突破的经皮移动皮肤,鼻Pallum和/或鼻子的皮肤。鉴于病变的性格和分布和细胞内酸快速杆菌的存在,我们假设通过血管和/或淋巴管途径发生病原体涂抹。诸如多核巨细胞和外周纤维化等原型肉芽肿的特征很少存在于受影响的猫鼬中。即使在坏死的区域中,均匀地发现酸快速的杆菌。 Mongoose Genome具有独特的缺失(RDIMON),其包括PPE68(RV3873)的部分编码区域,具有PE35的基因共操作。这些蛋白质可以影响宿主对分枝杆菌感染的细胞免疫应答,并且仍然不确定这种缺失如何有助于观察到的病理模式。 M.带状野牙的Mungi感染的特点是独特的传播和曝光路线,以及随附的病理特征,提供了增加我们对宿主病原体系统对MTC发病机制的理解的机会。

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